Phase IIa Clinical Trial of Curcumin for the Prevention of Colorectal Neoplasia

Carroll, Robert E.; Benya, Richard V.; Turgeon, D. Kim; Vareed, Shaiju K.; Neuman, Malloree; Rodríguez, Luz M.; Kakarala, Madhuri; Carpenter, Philip M.; McLaren, Christine E.; Meyskens, Frank L.; Brenner, Dean E.

doi:10.1158/1940-6207.capr-10-0098

Cited by 450 publications

(319 citation statements)

References 54 publications

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“…The continuously growing list of natural compounds ( Table 1) that modulate epigenetic mechanisms shows the great interest in this exciting field and clinical trials performed with several of these compounds (Table 2) confirm their efficiency. Quercetin, fisetin, myricetin Lee et al (2005) Caffeic acid Lee and Zhu (2006) Chlorogenic acid Cadaveric renal transplantation 480 mg; 1-2/day 9 30 days 43 Improved renal function, reduced neurotoxicity Shoskes et al (2005) Cardiovascular disease 500 mg/day 9 7 days 10 Decreased serum lipid peroxidase (33%), increased HDL cholesterol (29%), decreased total serum cholesterol (12%) Soni and Kuttan (1992) Chronic anterior uveitis 375 mg; 39/day 9 84 days 32 86% decrease in chronic anterior uveitis Lal et al (1999) Crohn's disease 360 mg; 3/day 9 30 days; 4 for 60 days 5 Improved symptoms Holt et al (2005) CRC 36-180 mg/day 9 120 days 15 Lowered GST Sharma et al (2001) CRC 450-3,600 mg/day 9 120 days 15 Lowered inducible serum PGE2 levels Sharma et al (2004) CRC 450-3,600 mg/day 9 7 days 12 Decreased M1G DNA adducts Garcea et al (2005) Colon cancer 10 g (n = 6) and 12 g (n = 6) 12 Pharmacokinetics Vareed et al (2008) CRC, ACF 2 g or 4 g/day for 30 days 44 A significant 40% reduction in ACF number occurred with the 4 g dose (P \ 0.005), whereas ACF were not reduced in the 2 g group Carroll et al (2011) External cancerous 1% ointment for several months 62 Reduction in smell in 90% patients, reduction of itching in all cases, dry lesions in 70% patients, reduction in lesion size and pain in 10% patients Kuttan et al (1987) Bundy et al (2004) Liver metastasis 450-3,600 mg/day 9 7 day 12 Low bioavailability Garcea et al (2004) (Fig. 2).…”

Section: Effect Of Other Natural Compounds On Epigeneticsmentioning

confidence: 98%

Epigenetic changes induced by curcumin and other natural compounds

et al. 2011

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Epigenetic regulation, which includes changes in DNA methylation, histone modifications, and alteration in microRNA (miRNA) expression without any change in the DNA sequence, constitutes an important mechanism by which dietary components can selectively activate or inactivate gene expression. Curcumin (diferuloylmethane), a component of the golden spice Curcuma longa, commonly known as turmeric, has recently been determined to induce epigenetic changes. This review summarizes current knowledge about the effect of curcumin on the regulation of histone deacetylases, histone acetyltransferases, DNA methyltransferase I, and miRNAs. How these changes lead to modulation of gene expression is also discussed. We also discuss other nutraceuticals which exhibit similar properties. The development of curcumin for clinical use as a regulator of epigenetic changes, however, needs further investigation to determine novel and effective chemopreventive strategies, either alone or in combination with other anticancer agents, for improving cancer treatment.

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Section: Effect Of Other Natural Compounds On Epigeneticsmentioning

confidence: 98%

Epigenetic changes induced by curcumin and other natural compounds

et al. 2011

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“…27 Although the therapeutic activities of Cur demonstrate its potential in cancer therapy, the issue of water insolubility greatly limits its further application, such as in drug formulation.…”

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confidence: 99%

Codelivery of SH-aspirin and curcumin by mPEG-PLGA nanoparticles enhanced antitumor activity by inducing mitochondrial apoptosis

Zhou¹,

Duan²,

Zeng³

et al. 2015

IJN

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Natural product curcumin (Cur) and H 2 S-releasing prodrug SH-aspirin (SH-ASA) are potential anticancer agents with diverse mechanisms, but their clinical application prospects are restricted by hydrophobicity and limited efficiency. In this work, we coencapsulated SH-ASA and Cur into methoxy poly(ethylene glycol)-poly (lactide-coglycolide) (mPEG-PLGA) nanoparticles through a modified oil-in-water single-emulsion solvent evaporation process. The prepared SH-ASA/Cur-coloaded mPEG-PLGA nanoparticles had a mean particle size of 122.3±6.8 nm and were monodispersed (polydispersity index =0.179±0.016) in water, with high drug-loading capacity and stability. Intriguingly, by treating with SH-ASA/Cur-coloaded mPEG-PLGA nanoparticles, obvious synergistic anticancer effects on ES-2 and SKOV3 human ovarian carcinoma cells were observed in vitro, and activation of the mitochondrial apoptosis pathway was indicated. Our results demonstrated that SH-ASA/Cur-coloaded mPEG-PLGA nanoparticles could have potential clinical advantages for the treatment of ovarian cancer.

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“…Curcumin was well tolerated at both doses. 44 In advanced pancreatic cancer, curcumin was found to be safe and well tolerated in a phase II clinical trial in which 25 patients were given 8 g of curcumin per day orally until disease progression. No toxicities associated with curcumin administration were reported in the patients.…”

Section: Curcuminoidsmentioning

confidence: 99%

Plant-derived anticancer agents: a promising treatment for bone metastasis

Juàrez¹

2014

BoneKEy Reports

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Bone metastasis is a very frequent complication of advanced cancer, and it remains an incurable disease. Current therapies that have been approved for the treatment of bone metastases delay the occurrence of skeletal-related events and can extend the patient's lifespan by a few years. However, they will not cure or cause the regression of established bone metastases, and new side effects are emerging after prolonged treatment. Thus, new therapies are severely needed. There are compelling evidences from in vitro and in vivo preclinical studies that support the use of compounds derived from plants to treat several forms of cancers including bone metastasis. More than 25% of the drugs used during the past 20 years were directly derived from plants, whereas another 25% are chemically altered natural products. Still, only 5-15% of the B250 000 higher plants have ever been investigated for bioactive compounds. There is a growing interest for the study of anticancer drugs with relatively low side effects that target specific key signaling pathways that control the establishment and progression of the cancer metastasis. Therefore, further studies are needed to identify new natural compounds with high efficiency in cancer prevention and treatment. Extensive reviews about plant-derived agents and their use in cancer have been published, but none when it comes to the treatment of bone metastases. Only a few of these compounds have been evaluated for the treatment of bone metastasis; here we describe some of the most prominent ones that are having the potential to reach the clinic soon.

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Phase IIa Clinical Trial of Curcumin for the Prevention of Colorectal Neoplasia

Cited by 450 publications

References 54 publications

Epigenetic changes induced by curcumin and other natural compounds

Epigenetic changes induced by curcumin and other natural compounds

Codelivery of SH-aspirin and curcumin by mPEG-PLGA nanoparticles enhanced antitumor activity by inducing mitochondrial apoptosis

Plant-derived anticancer agents: a promising treatment for bone metastasis

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